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556 American Family Physician www.aafp.org/afp Volume 87, Number 8 ◆ April 15, 2013
Updated Guidelines on Outpatient AnticoagulationPATRICIA WIGLE, PharmD, BCPS, and BRADLEY HEIN, PharmD, University of Cincinnati James L. Winkle College of Pharmacy, Cincinnati, Ohio
HANNA E. BLOOMFIELD, MD, MPH, University of Minnesota and Minneapolis VA Medical Center, Minneapolis, Minnesota
MATTHEW TUBB, MD, PhD, The Christ Hospital/University of Cincinnati Family Medicine Residency Program, Cincinnati, Ohio
MICHAEL DOHERTY, PharmD, BCACP, University of Cincinnati James L. Winkle College of Pharmacy, Cincinnati, Ohio
Warfarin (Coumadin), unfrac- tionated heparin, and low-molecular-weight heparin (LMWH) are commonly
used for the prevention and treatment of dis-orders such as systemic embolism associated with atrial fibrillation, stroke, and venous thromboembolism (VTE). LMWH allows for the initiation of anticoagulation therapy on an outpatient basis.
After decades during which warfarin was the only oral anticoagulation option, newer anticoagulants have the potential to change the management of coagulation disorders. This article focuses on the indications for and the goals and duration of anticoagula-tion therapy; describes methods to initiate therapy; and provides guidance on monitor-ing. Most of the recommendations are based
on the American College of Chest Physicians (ACCP) evidence-based clinical practice guidelines (Table 1).1
Warfarin, Heparin, and Heparin Analogues WARFARIN
The anticoagulant effect of warfarin results from the inhibition of the cyclic interconver-sion of vitamin K in the liver. The reduced form of vitamin K is necessary for the car-boxylation of the terminal regions of the vitamin K proteins, factors II, VII, IX, and X.1 Without carboxylation, these vitamin K–dependent clotting factors do not become activated. Warfarin, similar in structure to vitamin K, interferes with the cyclic res-toration of reduced levels of vitamin K. Therefore, warfarin indirectly reduces the
The American College of Chest Physicians provides recommendations for the use of anticoagulant medications for several indications that are important in the primary care setting. Warfarin, a vitamin K antagonist, is recommended for the treatment of venous thromboembolism and for the prevention of stroke in persons with atrial fibrillation, atrial flutter, or valvular heart disease. When warfarin therapy is initiated for venous thromboembolism, it should be given the first day, along with a heparin product or fondaparinux. The heparin product or fondaparinux should be continued for at least five days and until the patient’s international normalized ratio is at least 2.0 for two con-secutive days. The international normalized ratio goal and duration of treatment with warfarin vary depending on indication and risk. Warfarin therapy should be stopped five days before major surgery and restarted 12 to 24 hours postoperatively. Bridging with low-molecular-weight heparin or other agents is based on balancing the risk of throm-boembolism with the risk of bleeding. Increasingly, self-testing is an option for selected patients on warfarin therapy. The ninth edition of the American College of Chest Physicians guidelines, published in 2012, includes a discussion of anticoagulants that have gained approval from the U.S. Food and Drug Administration since publication of the eighth edition in 2008. Dabigatran and apixaban are indicated for the prevention of systemic embolism and stroke in persons with nonvalvular atrial fibrillation. Rivaroxaban is indicated for the prevention of deep venous thrombosis in patients undergoing knee or hip replacement surgery, for treatment of deep venous thrombosis and pulmonary embolism, for reducing the risk of recurrent deep venous thrombosis and pulmonary embolism after initial treatment, and for prevention of systemic embolism in patients with nonvalvular atrial fibrillation. (Am Fam Physician. 2013;87(8):556-566. Copyright © 2013 American Academy of Family Physicians.)
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April 15, 2013 ◆ Volume 87, Number 8 www.aafp.org/afp American Family Physician 557
synthesis of these clotting factors. The anticoagulant effects of warfarin are delayed for several days after dos-ing changes, including therapy initiation. This is because of the variable half-lives of previously formed circulating clotting factors. Carboxylation inhibition can also result in a paradoxical increased risk of clotting when warfarin
is initiated because of decreased levels of the vitamin K–dependent anticoagulant proteins C and S.1
Indications. Indications for initiating warfarin are listed in Table 2.1 In persons with nonvalvular atrial fibrillation, clinicians often base the decision to start warfarin or LMWH on clinical risk estimates, such as the
Table 1. Key Changes in the Ninth Edition of the American College of Chest Physicians Guidelines on Outpatient Management of Anticoagulation Therapy
Medication Recommendation Implication for practice
Dabigatran (Pradaxa)
Recommended over warfarin (Coumadin) in patients with nonvalvular atrial fibrillation who do not have severe renal impairment (grade 2B)
Simplification of anticoagulation management: no need for frequent dosage adjustments, INR monitoring
Caution: no antidote for reversal
LMWH Outpatients with solid tumors, additional risk factors for deep venous thrombosis, and low bleeding risk should receive prophylactic doses of LMWH (grade 2B)
—
Vitamin K Revised recommendations for treatment of patients with supratherapeutic INRs who do not have significant bleeding
For patients with an INR between 4.5 and 10, routine use of vitamin K is not recommended (grade 2B)
For patients with an INR greater than 10 without significant bleeding, oral vitamin K is recommended (grade 2C)
Advocating more judicious and conservative use of vitamin K
Warfarin Warfarin therapy at 10 mg daily for two days may be initiated in healthy outpatients with acute thromboembolism (grade 2C)
Helps to achieve therapeutic INR sooner and decreases the number of LMWH doses needed
Patients at high risk of bleeding may be better suited for traditional dosing
Caution: check INR after two or three doses
If the patient was previously stable on warfarin and presents with an isolated INR of 0.5 or less above or below therapeutic range, the current dosage should be continued and the patient retested in one to two weeks (grade 2C)
Patients taking the same dose for at least three consecutive months are considered stable
Physicians have the option of waiting until two consecutive INRs are outside the desired therapeutic range before changing the dose in previously stable patients who have not experienced a change in health, diet, or medication status; this method has not been associated with increased risk of bleeding or thromboembolism in observational studies
Minimizes burdens of unnecessary testing and dose adjustment
In previously stable patients with a single INR below the therapeutic range, routine heparin bridging is not recommended (grade 2C)
Applies to patients with two previous stable INRs
INRs should be checked in one to two weeks to verify return to desired range
Bridging may need to be considered in high-risk patients or in patients with continued subtherapeutic INRs
Minimizing unnecessary heparin bridging will save money and decrease patient burden
INR should be monitored up to every 12 weeks in patients who are stable, which is defined as having at least three months of consistent results with no need to adjust warfarin dosing (grade 2B)
Substantially lengthening the monitoring interval in stable patients (from every four weeks to up to every 12 weeks) will save money and enhance patient quality of life
Candidates for extended monitoring should demonstrate the ability to be compliant with medication and to recognize the signs and symptoms of over- and underanticoagulation
Caution: physicians should be alert for health or medication changes that may warrant more frequent monitoring
NOTE: Grade 1 recommendations are strong recommendations that can be applied to most patients; grade 2 recommendations are weaker recom-mendations. Grade A recommendations are supported by high-quality evidence, grade B recommendations are based on randomized clinical trials with methodological flaws or inconsistent results, and grade C recommendations are based on weaker evidence.
INR = international normalized ratio; LMWH = low-molecular-weight heparin.
Information from reference 1.
Table 2. Indications for and Goals and Duration of Warfarin Therapy
Indication (ACCP recommendation grade) Target INR (range) Duration of therapy (ACCP recommendation grade)
DVT of the leg or PE*
First episode (1B) 2.5 (2.0 to 3.0) First episode of proximal DVT or PE due to surgery
3 months recommended over short-term use (1B), longer use (1B), or extended therapy (1B)
First episode of proximal DVT or PE due to a reversible risk factor
3 months preferred over short-term use (1B), longer use (1B), or extended therapy (1B or 2B, depending on bleeding risk†)
First episode of distal DVT due to surgery or a reversible risk factor
3 months preferred over short-term use (2C), longer use (1B), or extended therapy (1B)
First episode of idiopathic proximal DVT or PE
Low or moderate bleeding risk†: extended use recommended over 3 months (2B); high bleeding risk†: 3 months recommended over extended use (1B for DVT; 1B for PE)
First episode of idiopathic distal DVT
3 months recommended over extended use (1B or 2B, depending on bleeding risk†)
Cancer (1B) 2.5 (2.0 to 3.0) Active cancer and PE
Low-molecular-weight heparin preferred over warfarin (Coumadin)
Extended use recommended (1B or 2B, depending on bleeding risk†)
Antiphospholipid antibody (2B) 2.5 (2.0 to 3.0) Antiphospholipid antibody and history of arterial or venous thrombosis
Extended use with target INR of 2.5 recommended over higher range of 3.0 to 4.5 (2B)
Second episode (1B) 2.5 (2.0 to 3.0) Two episodes of unprovoked DVT or PE
Low (1B) or moderate bleeding risk†: extended therapy (2B)
High bleeding risk†: 3 months (2B)
Atrial fibrillation or flutter
Intermediate‡ to high§ risk of stroke|| (1B)
2.5 (2.0 to 3.0) Indefinite
Elective cardioversion (1B) 2.5 (2.0 to 3.0) 3 weeks before if scheduled and for 4 weeks after conversion (1B/2C)
Mitral stenosis (1B) 2.5 (2.0 to 3.0) Indefinite
After stent placement and high risk of stroke (2C)
2.5 (2.0 to 3.0) Bare-metal stent (1 month) and drug-eluting stent (3 to 6 months) as triple therapy with clopidogrel (Plavix) and aspirin (2C)
After initial triple therapy, continue warfarin and a single antiplatelet agent until 12 months after stent placement (2C)
After 12 months: warfarin alone (2C)
Coronary heart disease
High-risk patients with myocardial infarction without a stent¶ (1B)
2.5 (2.0 to 3.0) with low-dose aspirin, 75 to 100 mg daily
3 months
High-risk patients with myocardial infarction and after stent placement¶ (2C)
2.5 (2.0 to 3.0) Bare-metal stent: triple therapy with warfarin, low-dose aspirin, and clopidogrel in month 1; combination of warfarin with single antiplatelet agent in months 2 and 3
Drug-eluting stent: triple therapy with warfarin, low-dose aspirin, and clopidogrel for 3 to 6 months
Valvular heart disease
Rheumatic mitral valve disease (1A if with atrial fibrillation or a history of systemic embolism; 1A if history of atrial thrombus; 2C if normal sinus rhythm and atrial diameter > 55 mm)
2.5 (2.0 to 3.0) Long-term
continued
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CHADS2 score, which assigns one point each for conges-tive heart failure, hypertension, age 75 years and older, and diabetes mellitus, and two points for prior ischemic stroke or transient ischemic attack.1 For persons with a CHADS2 score of 2 or higher, the ACCP guidelines rec-ommend oral anticoagulation, and for persons with a score of 1, the guidelines recommend individualization of therapy and suggest oral anticoagulation rather than a combination of aspirin and clopidogrel (Plavix).1
Dosing. Patients on warfarin therapy should be treated using a systematic process to optimize effectiveness and minimize adverse effects. Health care professionals skilled in the initiation and assessment of therapy and adjust-ments in dosing can dramatically influence outcomes.2,3
When warfarin is initiated, the international normal-ized ratio (INR) may begin to respond after two to three days because of the depletion of factor VII. During this initial period, the patient can enter a hypercoagulable state caused by warfarin’s effects on proteins C and S.1 Heparin or LMWH should be administered with warfa-rin initiation and continued until the INR has been in the targeted therapeutic range for a minimum of 24 hours.
Initial dosing of warfarin can vary depending on indi-vidual patient factors (e.g., age, bleeding risk, medication compliance history) and anticipated drug interactions.
In most patients, warfarin should be initiated as a main-tenance dosage of 5 mg daily. Older patients and persons with liver disease, poor nutritional status, or heart failure may require lower initiation dosages.1 For persons who are healthy enough to be treated as outpatients, the ACCP guidelines provide an alternative warfarin initiation dos-age of 10 mg daily for the first two days of therapy, rather than the anticipated maintenance dosage.1
After baseline INR is determined, the next INR can be obtained after the patient has received two or three doses. Then, the frequency of INR monitoring decreases to twice weekly until the INR is within the therapeu-tic range, then weekly, every other week, and finally monthly.1 The ACCP guidelines allow clinicians to con-sider INR monitoring up to every 12 weeks in patients who are stable (defined as having at least three months of consistent results with no need to adjust warfarin dosing). If a patient’s INR becomes subtherapeutic or supratherapeutic, the frequency of monitoring should
Table 2. Indications for and Goals and Duration of Warfarin Therapy (continued)
Indication (ACCP recommendation grade) Target INR (range) Duration of therapy (ACCP recommendation grade)
Valvular heart disease (continued)
Mechanical prosthetic heart valves (aortic position [2C over low-range INR and 1B over high-range INR]; mitral position [2C over low-range INR])
Bileaflet or tilting-disk valves: 2.5 (2.0 to 3.0) in the aortic position, and 3.0 (2.5 to 3.5) in the mitral position
Long-term
Recommended to use aspirin, 50 to 100 mg daily, with mechanical aortic or mitral valve and low bleeding risk
Bioprosthetic valves in the mitral position (2C)
2.5 (2.0 to 3.0) 3 months after insertion
Prevention of venous thromboembolism for orthopedic surgery
Elective total hip or knee replacement and hip fracture surgery (1B)
2.5 (2.0 to 3.0) 10 to 14 days minimum (1B)
35 days for major orthopedic surgery (2B)
Warfarin is second-line agent to low-molecular-weight heparin for total hip or total knee arthroplasty (2C)
NOTE: Grade 1 recommendations are strong recommendations that can be applied to most patients; grade 2 recommendations are weaker recom-mendations. Grade A recommendations are supported by high-quality evidence, grade B recommendations are based on randomized clinical trials with methodological flaws or inconsistent results, and grade C recommendations are based on weaker evidence.
ACCP = American College of Chest Physicians; CHADS2 = congestive heart failure, hypertension, age ≥ 75 years, diabetes mellitus, prior ischemic stroke or transient ischemic attack (doubled); DVT = deep venous thrombosis; INR = international normalized ratio; PE = pulmonary embolism.
*—Recommendation to start warfarin on first day of treatment with a parenteral anticoagulant (unfractionated or low-molecular-weight heparin, or fondaparinux [Arixtra]); 1B.†—Risk factors that increase a patient’s bleeding risk include advanced age, active gastric or duodenal ulcer, recent gastrointestinal bleeding, history of stroke, myocardial infarction, diabetes, and several laboratory abnormalities (e.g., elevated creatinine level, low platelet count, low hematocrit level).‡—Defined as CHADS2 score of 1. §—Defined as CHADS2 score of 2 or greater.||—Of note, in patients with a CHADS2 score of 0, aspirin (75 to 325 mg daily) is recommended as an option; 2B.¶—Patients with large anterior wall myocardial infarction who have left ventricular thrombus or who are at high risk of left ventricular thrombus (ejection fraction < 40 percent or anteroapical wall motion abnormality); 1B.
Information from reference 1.
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560 American Family Physician www.aafp.org/afp Volume 87, Number 8 ◆ April 15, 2013
be increased until it stabilizes again. The ACCP provides recommendations for managing supratherapeutic INRs (Table 3).1
Patients taking warfarin in the evening can adjust their dosing based on that day’s INR results. If the INR is not within the desired therapeutic range after exclud-ing explanatory factors, a 5 to 20 percent increase or decrease in the total weekly dosage is required.4-6 Patients should be provided with the simplest regimen to achieve the new total weekly dosage.
Drug, Food, and Disease State Interactions. Warfarin is subject to many drug-drug, drug-food, and drug– disease state interactions. eTable A lists selected drug-drug interactions that are considered highly likely to potentiate or inhibit the effects of warfarin.
Some medications, such as amiodarone and rifampin, can impact a patient’s INR long after the medication is discontinued.1,7,8 A patient taking a medication with higher interaction potential, such as metronidazole (Flagyl), should be monitored more frequently.9 Depend-ing on the patient and the medication, a prophylactic reduction in warfarin dosage may also be advised.
Foods with high vitamin K concentrations, such as leafy green vegetables, have the potential to partially reverse the anticoagulation effects of warfarin.8 A consistent diet is more important than limiting dietary vitamin K.1
Medical conditions such as diarrhea, heart failure, fever, hyperthyroidism, and liver disease can potentiate warfarin’s effects. Conversely, conditions such as hypo-thyroidism can decrease the expected effects of warfa-rin.1 Genetic factors can predispose patients to reduced warfarin requirements, as well as warfarin resistance. Although there is a small subset of patients who may have unexpected responses to warfarin, it is not currently rec-ommended that patients undergo genetic testing.1
UNFRACTIONATED HEPARIN
Unfractionated heparin is a mixture of glycosaminogly-cans that works by binding to antithrombin to inactivate thrombin (factor IIa) and factor Xa.1 It also prevents the growth and potential propagation of clots. Considerations for parenteral medications are provided in eTable B.
Beyond increased bleeding risk, unfractionated hep-arin is associated with other adverse effects, such as heparin-induced thrombocytopenia. Heparin-induced throm bo cytopenia should be suspected if a patient’s platelet count decreases by at least 50 percent, or is less than 150 × 103 per µL after initiation of heparin. This generally occurs five to 14 days after initiation, and can occur after heparin is discontinued.
LOW-MOLECULAR-WEIGHT HEPARIN
Two LMWHs, dalteparin (Fragmin) and enoxapa-rin (Lovenox), are commonly used in clinical practice. LMWH is derived from unfractionated heparin and has an increased affinity for factor Xa relative to thrombin.1 LMWH, which is given subcutaneously, has predictable absorption and degree of anticoagulation. Monitoring with measurement of anti–factor Xa levels is not rou-tinely recommended, but is potentially useful in certain situations in which predictability of the degree of antico-agulation may be altered, such as changes in pharmacoki-netics and pharmacodynamics (e.g., obesity, pregnancy) and accumulation (e.g., older age, kidney disease). In the outpatient setting, the usefulness of laboratory test-ing is limited to the assessment of bleeding events and therapeutic failures. It may also be of value to assess lev-els infrequently during the course of long-term therapy (i.e., when LMWH is used for more than just bridging therapy). Although LMWH has a similar bleeding risk and lower heparin-induced thrombocytopenia risk
Table 3. Management of Supratherapeutic INRs in Patients Without Significant Bleeding
INR Management Vitamin K dosing
Greater than goal INR, but < 4.5
Option 1: Decrease or hold dosage, increase frequency of monitoring, and resume at lower dosage once INR is within the therapeutic range
Option 2: May continue current dosage if INR is minimally elevated (0.5 or less above therapeutic range in a previously stable patient; grade 2C)
Not applicable
4.5 to 10 Hold next one or two doses, increase frequency of monitoring, and resume at lower dosage once INR is within the therapeutic range
No vitamin K (grade 2B)
Not applicable
> 10 Hold warfarin (Coumadin) and administer vitamin K (grade 2C), increase frequency of monitoring, repeat vitamin K as necessary, and resume warfarin at an appropriate dosage when INR is within the therapeutic range
2.5 to 5 mg orally as one dose
NOTE: Grade 1 recommendations are strong recommendations that can be applied to most patients; grade 2 recommendations are weaker recom-mendations. Grade A recommendations are supported by high-quality evidence, grade B recommendations are based on randomized clinical trials with methodological flaws or inconsistent results, and grade C recommendations are based on weaker evidence.
INR = international normalized ratio.
Information from reference 1.
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compared with unfractionated heparin, a patient with a history of heparin-induced thrombocytopenia should not take LMWH.1
FONDAPARINUX
Fondaparinux (Arixtra) is a synthetic analogue of hepa-rin. Unlike LMWH, fondaparinux is specific only to fac-tor Xa and has no effect on thrombin formation. Like LMWH, fondaparinux is given subcutaneously and has predictable absorption and degree of anticoagulation. The ACCP guidelines recommend fondaparinux for general surgical prophylaxis in patients who have con-traindications to LMWH.1
There are few data on the monitoring of fondaparinux. Anti–factor Xa levels can be used as long as fondaparinux (and not LMWH) is the reference standard in the assay.1 Although the bleeding risk is similar to unfractionated heparin and LMWH, there is little heparin-induced thrombocytopenia risk with fondaparinux.
Bridging Unfractionated Heparin, LMWH, or Fondaparinux to WarfarinIn the treatment of VTE and pulmonary embolism, the parenteral anticoagulant should be overlapped with war-farin for a minimum of five days. In most cases, warfa-rin can be initiated on day 1, after the first dose of the parenteral agent has been given. Warfarin should not be initiated alone, and the parenteral anticoagulant should not be discontinued until the INR is in the therapeutic range for two consecutive days.
Depending on the patient’s risk of thromboembolism and bleeding, bridging should occur when a patient’s oral anticoagulation therapy needs to be interrupted (eTable C). Interruption is common in patients undergo-ing surgery. For most persons who are not having a minor procedure, warfarin will be stopped approximately five days before surgery and restarted 12 to 24 hours post-operatively. LMWH should be restarted approximately 24 hours after the procedure, and it may be prudent to wait 48 to 72 hours before resuming the medication for patients at high risk of bleeding or who are undergoing major surgery.1 Fondaparinux is not recommended for this indication.
For all warfarin indications, perioperative bridging is not indicated in patients at low risk of thromboembo-lism.1 For patients with a high risk of thromboembolism, bridging with a therapeutic dose of unfractionated hepa-rin or LMWH is indicated.1 The ACCP guidelines are less clear about how patients with a moderate risk of throm-boembolism should be treated.1 Clinicians need to bal-ance the individual’s risk of thromboembolism, based
on the medical history and surgical procedure, and risk of bleeding when determining what is optimal in persons in this moderate-risk category.
Newer AnticoagulantsThe effectiveness of warfarin is well-established; how- ever, it is a suboptimal anticoagulant because it requires frequent monitoring and dosage adjustments, and because of its potential for multiple drug-drug, drug-food, and drug–disease state interactions. It has a lengthy half-life and a delayed anticoagulant effect, and it often requires bridging therapy.
Since the approval of warfarin in 1954, no other oral option existed for patients who needed long-term anti-coagulation therapy. This changed in 2010 with the U.S. Food and Drug Administration (FDA) approval of the oral direct thrombin inhibitor dabigatran (Pradaxa), in 2011 with the FDA approval of the oral direct factor Xa inhibitor rivaroxaban (Xarelto), and again in 2012 with the FDA approval of the oral factor Xa inhibitor apixa-ban (Eliquis). Characteristics of these anticoagulants are provided in Tables 4 and 5.10-19
DABIGATRAN
Dabigatran is available as a fixed-dose medication for the prevention of systemic embolism and stroke in patients with nonvalvular atrial fibrillation.13 The ACCP guide-lines recommend dabigatran, 150 mg twice daily, over warfarin for this indication when dosed appropriately for the patient’s renal function.1 Dabigatran does not require monitoring, dosage adjustments, or overlap with inject-able anticoagulants such as heparin. Without applicable laboratory monitoring, there is no mechanism to estab-lish if a patient’s INR is subtherapeutic or suprathera-peutic. If the patient’s INR is supratherapeutic, there is no antidote for reversal. This can be problematic when determining the appropriate management in a patient who needs emergent surgery. The short half-life is poten-tially challenging when assessing the impact of noncom-pliance or missing the second daily dose. Limited data are available for patients with hepatic impairment and for patients who are obese. Thus, it is not acceptable to automatically consider all patients taking warfarin to be good candidates for dabigatran.
Adverse effects of dabigatran, 150 mg twice daily, com-pared with warfarin include dyspepsia (11.3 versus 5.8 percent; P < .001) and major gastrointestinal bleeding (1.51 versus 1.02 percent; P < .001). Dabigatran’s safety profile needs further evaluation.13
Elevated transaminase levels in the Randomized Eval-uation of Long-term Anticoagulation Therapy trial were
562 American Family Physician www.aafp.org/afp Volume 87, Number 8 ◆ April 15, 2013
Table 4. Characteristics of Newer Oral Anticoagulants
Characteristic Apixaban (Eliquis) Dabigatran (Pradaxa) Rivaroxaban (Xarelto)
Mechanism of action Direct factor Xa inhibitor Direct thrombin inhibitor Direct factor Xa inhibitor
FDA boxed warning/contraindications
FDA boxed warning: increased risk of stroke in patients with nonvalvular atrial fibrillation who discontinue apixaban without adequate continuous anticoagulation
Contraindications: active pathological bleeding; history of serious hypersensitivity reaction to apixaban
Use not recommended in patients with prosthetic heart valves or severe hepatic impairment; pregnant or breastfeeding patients
Contraindications: active pathological bleeding; history of serious hypersensitivity reaction to dabigatran; mechanical prosthetic heart valve
Use not recommended in patients with bioprosthetic heart valves; pregnant or breastfeeding patients
FDA boxed warning: increased risk of thrombotic events in patients with nonvalvular atrial fibrillation who discontinue rivaroxaban without adequate continuous anticoagulation; risk of epidural/spinal hematoma in patients receiving neuraxial anesthesia or in patients undergoing spinal puncture while taking rivaroxaban
Contraindications: active pathological bleeding; history of severe hypersensitivity reaction to rivaroxaban
Use not recommended in pregnant or breastfeeding patients
Indications Reduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillation
Reduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillation
Prevent DVT in patients undergoing knee or hip replacement surgeryReduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillationTreat DVT and pulmonary embolismReduce risk of recurrent DVT and pulmonary embolism after initial treatment
Usual dosage 5 mg twice daily2.5 mg twice daily if patient has at least 2 of the following:
age 80 years or older, body weight of 132 lb (60 kg) or less, or serum creatinine level of 1.5 mg per dL or higher
No data for patients on dialysis or with CrCl < 15 mL/min/ 1.73 m2 or patients with moderate hepatic impairment
Not recommended for patients with severe hepatic impairment2.5 mg twice daily if patient is on a strong dual inhibitor of
CYP3A4 and P-glycoprotein (e.g., ketoconazole, itraconazole [Sporanox], ritonavir [Norvir], clarithromycin [Biaxin]); avoid use of these drugs if patient is already taking 2.5 mg twice daily
150 mg twice daily CrCl 30 to 50 mL/min/1.73 m2 and concurrent use
of dronedarone (Multaq) or systemic ketoconazole: decrease dosage to 75 mg twice daily
CrCl 15 to 30 mL/min/1.73 m2: decrease dosage to 75 mg twice daily
CrCl < 30 mL/min/1.73 m2 and concurrent use of a P-glycoprotein inhibitor: avoid use
CrCl < 15 mL/min/1.73 m2: avoid use No data for patients on dialysis
DVT prophylaxis: 10 mg once daily DVT prophylaxis and CrCl < 30 mL/min/1.73 m2: avoid usePrevent stroke in patients with nonvalvular atrial fibrillation: 20 mg once dailyPrevent stroke in patients with nonvalvular atrial fibrillation and CrCl 15 to 50 mL/
min/1.73 m2: 15 mg once dailyPrevent stroke in patients with nonvalvular atrial fibrillation and CrCl < 15 mL/min/
1.73 m2: avoid useTreat DVT and pulmonary embolism or reduce risk of future DVT and pulmonary
embolism after initial treatment: 15 mg twice daily with food for 21 days, then 20 mg once daily for the remainder of the treatment interval (six months total) or for long-term risk reduction; avoid in patients with CrCl < 30 mL/min/1.73 m2
Half-life 12 hours (with repeat dosing) 12 to 17 hours 5 to 9 hours
Monitoring None recommended None recommended None recommended
Antidote None available None available None available
Drug interactions See “usual dosage” for dose modification informationAvoid use of strong dual inhibitor of CYP3A4 and P-glycoprotein
in patients taking apixaban, 2.5 mg twice dailyAvoid use of strong dual inducer of CYP3A4 and P-glycoprotein
(e.g., carbamazepine [Tegretol], phenytoin [Dilantin], rifampin, St. John’s wort)
Increased bleeding risk with certain medications (e.g., clopidogrel [Plavix], nonsteroidal anti-inflammatory drugs)
See “usual dosage” for dose modification information
Avoid concurrent use with P-glycoprotein inducers (e.g., rifampin)
Evaluate P-glycoprotein inhibitors individually*Increased bleeding risk with certain medications
(e.g., clopidogrel, nonsteroidal anti-inflammatory drugs)
See “usual dosage” for dose modification informationAvoid with combined P-glycoprotein inhibitor and CYP3A4 inhibitor
(e.g., ketoconazole, itraconazole, ritonavir, conivaptan [Vaprisol])Avoid with combined P-glycoprotein inducer and CYP3A4 inducer
(e.g., carbamazepine, phenytoin, rifampin, St. John’s wort) Increased bleeding risk with certain medications (e.g., clopidogrel, nonsteroidal
anti-inflammatory drugs)
Adverse effects Bleeding Bleeding, dyspepsia Bleeding
Impact of renal impairment
See “usual dosage” for dose modification information See “usual dosage” for dose modification information
See “usual dosage” for dose modification informationNote differences in recommendation for dosage adjustments in renal impairment
based on indication
Impact of hepatic impairment
See “usual dosage” for dose modification informationDosing recommendations for patients with moderate hepatic
impairment are not available
No specific recommendations are made regarding hepatic impairment
Limited information in this population
Avoid if moderate (Child-Pugh class B) or severe (Child-Pugh class C) hepatic impairment or with any hepatic disease associated with coagulopathy
Comments No objective way to monitor nonadherenceRefer to package labeling for information on conversion from
or to warfarin (Coumadin) or parenteral anticoagulants, and on intervention for surgery
Do not chew, break, open capsules; capsules must be dispensed in original container and not repackaged because of sensitivity to moisture
No objective way to measure nonadherenceNeed more information about use in patients under
and over ideal body weightRefer to package labeling for information on
conversion from or to warfarin or parenteral anticoagulants, and on intervention for surgery
Rivaroxaban should be stopped 24 hours before major surgeryDVT prophylaxis
The first dose should be initiated 6 to 10 hours after surgeryRecommended duration of therapy is 12 days for total knee replacement and
35 days for total hip replacementPrevent stroke in patients with atrial fibrillation
When transitioning from warfarin to rivaroxaban, give first dose of rivaroxaban when the international normalized ratio is less than 3
CrCl = creatinine clearance; CYP3A4 = cytochrome P450 3A4; DVT = deep venous thrombosis; FDA = U.S. Food and Drug Administration.
*—Amiodarone, clarithromycin, quinidine, and verapamil have been evaluated with dabigatran and do not require a dabigatran dosage adjustment, but should be used concurrently with caution. Other P-glycoprotein inhibitors should be evaluated on an individual basis.
Information from references 10 through 19.
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comparable to those seen with warfarin, and routine liver function test monitor-ing is not recommended.11,13 Because of the effects of renal function on dabigatran, baseline and periodic renal function moni-toring are recommended.
RIVAROXABAN
Rivaroxaban is indicated for prevention of deep venous thrombosis in patients under-going knee or hip replacement surgery, for treatment of deep venous thrombosis and pulmonary embolism, for reducing the risk of recurrent deep venous thrombo-sis and pulmonary embolism after initial treatment, and for prevention of systemic embolism in patients with nonvalvular atrial fibrillation. It is expected to prolong the activated partial thromboplastin time and increase anti–factor Xa levels; how-ever, the usefulness of monitoring has not been established. In four trials evaluating the role of rivaroxaban in the prevention of VTE in patients undergoing orthopedic surgery, rivaroxaban significantly reduced the primary outcome (total VTE and all-cause mortality) compared with enoxa-parin, without significantly increasing bleeding risk.14-19 In the ROCKET AF trial, rivaroxaban was shown to be noninferior to warfarin for the prevention of stroke or systemic embolism in patients with non-valvular atrial fibrillation.19 An important consideration in this trial is that in the war-farin arm, the time in therapeutic range was 55 percent, which is less than what is typi-cally reported by anticoagulation clinics.
Rivaroxaban has been studied for the treat-ment of acute coronary syndromes. Similar to dabigatran, baseline and periodic renal function monitoring are recommended.
APIXABAN
Similar to dabigatran, apixaban is also indi-cated for the prevention of systemic embo-lism and stroke in patients with nonvalvular atrial fibrillation. In the ARISTOTLE and AVERROES trials, apixaban reduced the primary outcome of ischemic stroke, hemorrhagic stroke, and systemic embo-lism compared with warfarin and aspirin,
Table 4. Characteristics of Newer Oral Anticoagulants
Characteristic Apixaban (Eliquis) Dabigatran (Pradaxa) Rivaroxaban (Xarelto)
Mechanism of action Direct factor Xa inhibitor Direct thrombin inhibitor Direct factor Xa inhibitor
FDA boxed warning/contraindications
FDA boxed warning: increased risk of stroke in patients with nonvalvular atrial fibrillation who discontinue apixaban without adequate continuous anticoagulation
Contraindications: active pathological bleeding; history of serious hypersensitivity reaction to apixaban
Use not recommended in patients with prosthetic heart valves or severe hepatic impairment; pregnant or breastfeeding patients
Contraindications: active pathological bleeding; history of serious hypersensitivity reaction to dabigatran; mechanical prosthetic heart valve
Use not recommended in patients with bioprosthetic heart valves; pregnant or breastfeeding patients
FDA boxed warning: increased risk of thrombotic events in patients with nonvalvular atrial fibrillation who discontinue rivaroxaban without adequate continuous anticoagulation; risk of epidural/spinal hematoma in patients receiving neuraxial anesthesia or in patients undergoing spinal puncture while taking rivaroxaban
Contraindications: active pathological bleeding; history of severe hypersensitivity reaction to rivaroxaban
Use not recommended in pregnant or breastfeeding patients
Indications Reduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillation
Reduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillation
Prevent DVT in patients undergoing knee or hip replacement surgeryReduce risk of stroke and systemic embolism in patients with nonvalvular atrial fibrillationTreat DVT and pulmonary embolismReduce risk of recurrent DVT and pulmonary embolism after initial treatment
Usual dosage 5 mg twice daily2.5 mg twice daily if patient has at least 2 of the following:
age 80 years or older, body weight of 132 lb (60 kg) or less, or serum creatinine level of 1.5 mg per dL or higher
No data for patients on dialysis or with CrCl < 15 mL/min/ 1.73 m2 or patients with moderate hepatic impairment
Not recommended for patients with severe hepatic impairment2.5 mg twice daily if patient is on a strong dual inhibitor of
CYP3A4 and P-glycoprotein (e.g., ketoconazole, itraconazole [Sporanox], ritonavir [Norvir], clarithromycin [Biaxin]); avoid use of these drugs if patient is already taking 2.5 mg twice daily
150 mg twice daily CrCl 30 to 50 mL/min/1.73 m2 and concurrent use
of dronedarone (Multaq) or systemic ketoconazole: decrease dosage to 75 mg twice daily
CrCl 15 to 30 mL/min/1.73 m2: decrease dosage to 75 mg twice daily
CrCl < 30 mL/min/1.73 m2 and concurrent use of a P-glycoprotein inhibitor: avoid use
CrCl < 15 mL/min/1.73 m2: avoid use No data for patients on dialysis
DVT prophylaxis: 10 mg once daily DVT prophylaxis and CrCl < 30 mL/min/1.73 m2: avoid usePrevent stroke in patients with nonvalvular atrial fibrillation: 20 mg once dailyPrevent stroke in patients with nonvalvular atrial fibrillation and CrCl 15 to 50 mL/
min/1.73 m2: 15 mg once dailyPrevent stroke in patients with nonvalvular atrial fibrillation and CrCl < 15 mL/min/
1.73 m2: avoid useTreat DVT and pulmonary embolism or reduce risk of future DVT and pulmonary
embolism after initial treatment: 15 mg twice daily with food for 21 days, then 20 mg once daily for the remainder of the treatment interval (six months total) or for long-term risk reduction; avoid in patients with CrCl < 30 mL/min/1.73 m2
Half-life 12 hours (with repeat dosing) 12 to 17 hours 5 to 9 hours
Monitoring None recommended None recommended None recommended
Antidote None available None available None available
Drug interactions See “usual dosage” for dose modification informationAvoid use of strong dual inhibitor of CYP3A4 and P-glycoprotein
in patients taking apixaban, 2.5 mg twice dailyAvoid use of strong dual inducer of CYP3A4 and P-glycoprotein
(e.g., carbamazepine [Tegretol], phenytoin [Dilantin], rifampin, St. John’s wort)
Increased bleeding risk with certain medications (e.g., clopidogrel [Plavix], nonsteroidal anti-inflammatory drugs)
See “usual dosage” for dose modification information
Avoid concurrent use with P-glycoprotein inducers (e.g., rifampin)
Evaluate P-glycoprotein inhibitors individually*Increased bleeding risk with certain medications
(e.g., clopidogrel, nonsteroidal anti-inflammatory drugs)
See “usual dosage” for dose modification informationAvoid with combined P-glycoprotein inhibitor and CYP3A4 inhibitor
(e.g., ketoconazole, itraconazole, ritonavir, conivaptan [Vaprisol])Avoid with combined P-glycoprotein inducer and CYP3A4 inducer
(e.g., carbamazepine, phenytoin, rifampin, St. John’s wort) Increased bleeding risk with certain medications (e.g., clopidogrel, nonsteroidal
anti-inflammatory drugs)
Adverse effects Bleeding Bleeding, dyspepsia Bleeding
Impact of renal impairment
See “usual dosage” for dose modification information See “usual dosage” for dose modification information
See “usual dosage” for dose modification informationNote differences in recommendation for dosage adjustments in renal impairment
based on indication
Impact of hepatic impairment
See “usual dosage” for dose modification informationDosing recommendations for patients with moderate hepatic
impairment are not available
No specific recommendations are made regarding hepatic impairment
Limited information in this population
Avoid if moderate (Child-Pugh class B) or severe (Child-Pugh class C) hepatic impairment or with any hepatic disease associated with coagulopathy
Comments No objective way to monitor nonadherenceRefer to package labeling for information on conversion from
or to warfarin (Coumadin) or parenteral anticoagulants, and on intervention for surgery
Do not chew, break, open capsules; capsules must be dispensed in original container and not repackaged because of sensitivity to moisture
No objective way to measure nonadherenceNeed more information about use in patients under
and over ideal body weightRefer to package labeling for information on
conversion from or to warfarin or parenteral anticoagulants, and on intervention for surgery
Rivaroxaban should be stopped 24 hours before major surgeryDVT prophylaxis
The first dose should be initiated 6 to 10 hours after surgeryRecommended duration of therapy is 12 days for total knee replacement and
35 days for total hip replacementPrevent stroke in patients with atrial fibrillation
When transitioning from warfarin to rivaroxaban, give first dose of rivaroxaban when the international normalized ratio is less than 3
CrCl = creatinine clearance; CYP3A4 = cytochrome P450 3A4; DVT = deep venous thrombosis; FDA = U.S. Food and Drug Administration.
*—Amiodarone, clarithromycin, quinidine, and verapamil have been evaluated with dabigatran and do not require a dabigatran dosage adjustment, but should be used concurrently with caution. Other P-glycoprotein inhibitors should be evaluated on an individual basis.
Information from references 10 through 19.
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respectively. There were also lower mortality rates in the apixaban group in both trials and a lower major bleeding rate in the apixaban group compared with warfarin in the ARISTOTLE trial.20,21
Five oral direct factor Xa inhibitors (i.e., betrixaban, TAK-442, darexaban, otamixaban, and edoxaban) are being assessed.18 AZD0837, which is comparable to dabi-gatran, and tecarfarin, which is similar to warfarin, are also under investigation.18
Patient Self-Testing Point-of-care monitors are typically used in primary care and anticoagulation clinics and have several advan-tages, including rapid INR acquisition and interpreta-tion. These monitors make it possible for patients to check their INRs at home, which is referred to as patient self-testing. Reassuring data exist for the effective use of patient self-testing in selected patients who demonstrate monitor competency. Decreased mortality, enhanced
Table 5. Comparison of Newer Oral Anticoagulants with Enoxaparin and Warfarin
Component Apixaban (Eliquis) vs. warfarin (Coumadin) Dabigatran (Pradaxa) vs. warfarin (Coumadin) Rivaroxaban (Xarelto) vs. warfarin (Coumadin) Rivaroxaban (Xarelto) vs. enoxaparin (Lovenox)
Advantages Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Lower bleeding risk compared with warfarin
Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Oral route of administration
At least as effective and possibly superior at reducing total venous thromboembolism without increasing major bleeding risk
Disadvantages Lack of long-term safety/effectiveness data
No antidote
No test for effectiveness or toxicity
Renal dosing
Twice-daily administration
U.S. Food and Drug Administration boxed warning for increased risk of thrombotic events when apixaban discontinued in patients with nonvalvular atrial fibrillation
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data (e.g., dyspepsia, hepatotoxicity, myocardial infarction)
No antidote
No test for effectiveness or toxicity
Packaging does not allow redistribution to pill boxes
Renal dosing
Twice-daily administration
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data
No antidote
No test for effectiveness or toxicity
Renal dosing
Noncompliance with medication potentially more harmful
U.S. Food and Drug Administration boxed warning for increased risk of thrombotic events when rivaroxaban discontinued in patients with nonvalvular atrial fibrillation
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data (e.g., hepatotoxicity)
No antidote
No test for effectiveness or toxicity
Cannot use in patients with moderate or severe hepatic impairment
More drug interactions
Clinical application By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, apixaban possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, dabigatran possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, rivaroxaban possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, relatively longer half-life, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
Oral administration makes it easier to allow for longer duration of deep venous thrombosis prophylaxis in patients undergoing orthopedic surgery
Information from references 10 through 19.
SORT: KEY RECOMMENDATIONS FOR PRACTICE
Clinical recommendationEvidence rating References
Patients taking warfarin (Coumadin) should be treated using systematic processes of care to optimize effectiveness and minimize adverse effects. Health care professionals skilled in the initiation and assessment of therapy and dosing adjustments can dramatically influence outcomes.
B 2, 3
In patients with atrial fibrillation and at least one other risk factor for stroke, newer agents (rivaroxaban [Xarelto] and dabigatran [Pradaxa]) that do not require frequent laboratory monitoring are as effective as warfarin for prevention of stroke or systemic embolism and have comparable risks of major bleeding.
A 11-19
Compared with usual clinic-based care, patient self-testing for international normalized ratios, with or without self-dosing of warfarin, is associated with significantly fewer deaths and thromboembolic complications without any increase in bleeding complications for a selected group of motivated patients who have completed appropriate training.
A 22-25
A = consistent, good-quality patient-oriented evidence; B = inconsistent or limited-quality patient-oriented evidence; C = consensus, disease-oriented evidence, usual practice, expert opinion, or case series. For information about the SORT evidence rating system, go to http://www.aafp.org/afpsort.xml.
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INR control, decreased thromboembolic events, and an improvement in patient satisfaction and quality of life have been demonstrated with patient self-testing, all without an increase in bleeding complications.22-24 In 2008, the Centers for Medicare and Medicaid Ser-vices expanded its patient self-testing coverage,25 which is outlined in eTable D. The cost of patient self-testing, which is similar to the cost of newer oral anticoagulants, can be significant without reimbursement; however, self-testing is not appropriate for all patients on warfa-rin therapy22-24 (eTable D).
Data Sources: A PubMed search was completed in Clinical Queries using the key terms outpatient, anticoagulation, warfarin, dabigatran, rivaroxaban, heparin, low-molecular-weight heparin, dalteparin, enoxa-parin, patient self-monitor, and INR. The search included meta-analyses, randomized controlled trials, clinical trials, clinical guidelines, and reviews. Also searched were the National Guideline Clearinghouse data-base, Essential Evidence Plus, UpToDate, the Cochrane database, and the Agency for Healthcare Research and Quality Clinical Guidelines and Evidence Reports. Search date: August 10, 2012.
The Authors
PATRICIA WIGLE, PharmD, BCPS, is an associate professor of pharmacy practice in the Division of Pharmacy Practice and Administrative Sciences at the University of Cincinnati (Ohio) James L. Winkle College of Phar-macy, and a clinical pharmacist in the outpatient anticoagulation clinic at West Chester (Ohio) Hospital.
BRADLEY HEIN, PharmD, is an associate professor of pharmacy practice in the Division of Pharmacy Practice and Administrative Sciences at the University of Cincinnati James L. Winkle College of Pharmacy, and a clini-cal pharmacist in internal medicine at The Christ Hospital in Cincinnati.
HANNA E. BLOOMFIELD, MD, MPH, is a professor of medicine at the Uni-versity of Minnesota, Minneapolis, and the co-chief of general internal medicine at the Minneapolis VA Medical Center.
MATTHEW TUBB, MD, PhD, is chief resident in The Christ Hospital/Univer-sity of Cincinnati Family Medicine Residency Program.
MICHAEL DOHERTY, PharmD, BCACP, is an assistant professor of phar-macy practice in the Division of Pharmacy Practice and Administrative Sci-ences at the University of Cincinnati James L. Winkle College of Pharmacy, and a clinical pharmacist in the outpatient anticoagulation clinic at West Chester Hospital.
Address correspondence to Patricia Wigle, PharmD, BCPS, University of Cincinnati James L. Winkle College of Pharmacy, 3225 Eden Ave., 304 Wherry Hall, Cincinnati, OH 45267 (e-mail: [email protected]). Reprints are not available from the authors.
Author disclosure: No relevant financial affiliations.
REFERENCES
1. Antithrombotic therapy and prevention of thrombosis, 9th ed: Ameri-can College of Chest Physicians evidence-based clinical practice guide-lines. Chest. 2012;141(suppl 2).
2. Hall D, Buchanan J, Helms B, et al. Health care expenditures and thera-peutic outcomes of a pharmacist-managed anticoagulation service ver-sus usual medical care. Pharmacotherapy. 2011;31(7):686-694.
3. Rudd KM, Dier JG. Comparison of two different models of anticoagula-
Table 5. Comparison of Newer Oral Anticoagulants with Enoxaparin and Warfarin
Component Apixaban (Eliquis) vs. warfarin (Coumadin) Dabigatran (Pradaxa) vs. warfarin (Coumadin) Rivaroxaban (Xarelto) vs. warfarin (Coumadin) Rivaroxaban (Xarelto) vs. enoxaparin (Lovenox)
Advantages Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Lower bleeding risk compared with warfarin
Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Fixed dose
Fewer drug and food interactions
No laboratory monitoring necessary
Oral route of administration
At least as effective and possibly superior at reducing total venous thromboembolism without increasing major bleeding risk
Disadvantages Lack of long-term safety/effectiveness data
No antidote
No test for effectiveness or toxicity
Renal dosing
Twice-daily administration
U.S. Food and Drug Administration boxed warning for increased risk of thrombotic events when apixaban discontinued in patients with nonvalvular atrial fibrillation
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data (e.g., dyspepsia, hepatotoxicity, myocardial infarction)
No antidote
No test for effectiveness or toxicity
Packaging does not allow redistribution to pill boxes
Renal dosing
Twice-daily administration
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data
No antidote
No test for effectiveness or toxicity
Renal dosing
Noncompliance with medication potentially more harmful
U.S. Food and Drug Administration boxed warning for increased risk of thrombotic events when rivaroxaban discontinued in patients with nonvalvular atrial fibrillation
Underweight patients and those with renal impairment may be at increased bleeding risk
Lack of long-term safety/effectiveness data (e.g., hepatotoxicity)
No antidote
No test for effectiveness or toxicity
Cannot use in patients with moderate or severe hepatic impairment
More drug interactions
Clinical application By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, apixaban possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, dabigatran possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
By alleviating the need for frequent dose titrations and laboratory monitoring, especially with therapy initiation and new drug additions or deletions, rivaroxaban possesses key clinical advantages compared with warfarin
Warfarin’s predictable adverse effect profile, once-daily administration, relatively longer half-life, reversibility with vitamin K, and ability to be monitored for sub- and supratherapeutic dosing provide reassurance for the clinician
Oral administration makes it easier to allow for longer duration of deep venous thrombosis prophylaxis in patients undergoing orthopedic surgery
Information from references 10 through 19.
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tion management services with usual medical care. Pharmacotherapy. 2010;30(4):330-338.
4. Garcia D, Regan S, Crowther M, Hughes RA, Hylek EM. Warfarin main-tenance dosing patterns in clinical practice: implications for safer anti-coagulation in the elderly population. Chest. 2005;127(6):2049-2056.
5. University of Michigan Cardiovascular Center. Anticoagulation manage-ment service for health professionals. Warfarin dose adjustment. http://www.med.umich.edu/cvc/prof/anticoag/dose.htm. Accessed Septem-ber 23, 2011.
6. Ebell MH. Evidence-based adjustment of warfarin (Coumadin) doses. Am Fam Physician. 2005;71(10):1979-1982.
7. Krajewski KC. Inability to achieve a therapeutic INR value while on con-current warfarin and rifampin. J Clin Pharmacol. 2010;50(6):710-713.
8. Nutescu E, Chuatrisorn I, Hellenbart E. Drug and dietary interactions of warfarin and novel oral anticoagulants: an update. J Thromb Throm-bolysis. 2011;31(3):326-343.
9. Thi L, Shaw D, Bird J. Warfarin potentiation: a review of the “FAB-4” significant drug interactions. Consult Pharm. 2009;24(3):227-230.
10. Eliquis (apixaban) tablets for oral use [prescribing information]. Princ-eton, N.J.: Bristol-Myers Squibb Company; 2012. http://packageinserts.bms.com/pi/pi_eliquis.pdf. Accessed January 23, 2013.
11. Pradaxa (dabigatran etexilate mesylate) capsules for oral use [prescrib-ing information]. Ridgefield, Conn.: Boehringer Ingelheim Pharmaceuti-cals; 2012. http://www.pradaxa.com. Accessed January 23, 2013.
12. Xarelto (rivaroxaban) tablets, for oral use [prescribing information]. Titusville, N.J.: 2011. http://www.xareltohcp.com/xarelto-prescribing-information.html. Accessed December 30, 2012.
13. Connolly SJ, Ezekowitz MD, Yusuf S, et al.; RE-LY Steering Commit-tee and Investigators. Dabigatran versus warfarin in patients with atrial fibrillation [published correction appears in N Engl J Med. 2010; 363(19):1877]. N Engl J Med. 2009;361(12):1139-1151.
14. Eriksson BI, Borris LC, Friedman RJ, et al.; RECORD1 Study Group. Riva-roxaban versus enoxaparin for thromboprophylaxis after hip arthro-plasty. N Engl J Med. 2008;358(26):2765-2775.
15. Kakkar AK, Brenner B, Dahl OE, et al.; RECORD2 Investigators. Extended
duration rivaroxaban versus short-term enoxaparin for the prevention of venous thromboembolism after total hip arthroplasty: a double-blind, randomised controlled trial. Lancet. 2008;372(9632):31-39.
16. Lassen MR, Ageno W, Borris LC, et al.; RECORD3 Investigators. Riva-roxaban versus enoxaparin for thromboprophylaxis after total knee arthroplasty. N Engl J Med. 2008;358(26):2776-2786.
17. Turpie AG, Lassen MR, Davidson BL, et al.; RECORD4 Investigators. Rivaroxaban versus enoxaparin for thromboprophylaxis after total knee arthroplasty (RECORD4): a randomised trial. Lancet. 2009;373 (9676):1673-1680.
18. Davis EM, Packard KA, Knezevich JT, Campbell JA. New and emerg-ing anticoagulant therapy for atrial fibrillation and acute coronary syn-drome. Pharmacotherapy. 2011;31(10):975-1016.
19. Patel MR, Mahaffey KW, Garg J, et al.; ROCKET AF Investigators. Riva-roxaban versus warfarin in nonvalvular atrial fibrillation. N Engl J Med. 2011;365(10):883-891.
20. Granger CB, Alexander JH, McMurray JJ, et al.; ARISTOTLE Committees and Investigators. Apixaban versus warfarin in patients with atrial fibril-lation. N Engl J Med. 2011;365(11):981-992.
21. Connolly SJ, Eikelboom J, Joyner C, et al.; AVERROES Steering Commit-tee and Investigators. Apixaban in patients with atrial fibrillation. N Engl J Med. 2011;364(9):806-817.
22. Gardiner C, Williams K, Mackie IJ, Machin SJ, Cohen H. Patient self-test-ing is a reliable and acceptable alternative to laboratory INR monitoring. Br J Haematol. 2005;128(2):242-247.
23. Matchar DB, Jacobson A, Dolor R, et al.; THINRS Executive Commit-tee and Site Investigators. Effect of home testing of international nor-malized ratio on clinical events [published correction appears in N Engl J Med. 2011;364(1):93]. N Engl J Med. 2010;363(17):1608-1620.
24. Garcia-Alamino JM, Ward AM, Alonso-Coello P, et al. Self-monitoring and self-management of oral anticoagulation. Cochrane Database Syst Rev. 2010;(4):CD003839.
25. Centers for Medicare and Medicaid Services. CMS Manual System. Pub 100-04 Medicare claims processing. Prothrombin time (PT/INR) moni-toring for home anticoagulation management. https://www.cms.gov/transmittals/downloads/R1562CP.pdf. Accessed August 29, 2011.
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eTable A. Selected Warfarin Drug-Drug Interactions
Potentiate the effects of warfarin (Coumadin)*
Antimicrobials
Ciprofloxacin (Cipro)
Clarithromycin (Biaxin)
Erythromycin
Isoniazid
Metronidazole (Flagyl)
Triazole antifungals
Trimethoprim/sulfamethoxazole (Bactrim, Septra)
Cardiovascular
Amiodarone
Diltiazem
Fibric acid derivatives
Propafenone (Rythmol)
Statins
*—Multiple medications increase bleeding risk because of antiplatelet activity (e.g., aspirin, salicylates, nonsteroidal anti-inflammatory drugs, heparin).†—Corticosteroids and phenytoin have variable effects on international normalized ratio.
Information from:
Antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians evidence-based clinical practice guidelines. Chest. 2012;141(suppl 2).
Thi L, Shaw D, Bird J. Warfarin potentiation: a review of the “FAB-4” significant drug interactions. Consult Pharm. 2009;24(3):227-230.
Shirolkar SC, Fiuzat M, Becker RC. Dronedarone and vitamin K antagonists: a review of drug-drug interactions. Am Heart J. 2010;160(4):577-582.
Krajewski KC. Inability to achieve a therapeutic INR value while on concurrent warfarin and rifampin. J Clin Pharmacol. 2010;50(6):710-713.
Nutescu E, Chuatrisorn I, Hellenbart E. Drug and dietary interactions of warfarin and novel oral anticoagulants: an update. J Thromb Thrombolysis. 2011;31(3):326-343.
Decrease the effects of warfarin
Antimicrobials
Griseofulvin
Rifampin
Central nervous system drugs
Barbiturates
Carbamazepine (Tegretol)
Chlordiazepoxide (Librium)
Trazodone
Complementary and alternative medicine products
American ginseng
Coenzyme Q10
St. John’s wort
Miscellaneous
Cholestyramine (Questran)
Corticosteroids†Mercaptopurine
Phenytoin†
Potentiate the effects of warfarin* (continued)
Complementary and alternative medicine products
Cranberry juice
Danshen
Fish oil
Ginkgo biloba
Red yeast rice
Miscellaneous
Acetaminophen (dosages ≥ 1.3 g daily)
Alcohol (acute ingestion)
Cimetidine (Tagamet)
Corticosteroids†Levothyroxine
Omeprazole (Prilosec)
Paroxetine (Paxil)
Phenytoin (Dilantin)†
BONUS DIGITAL CONTENT
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eTable B. Unfractionated Heparin, LMWH, and Fondaparinux for Outpatient Treatment of Venous Thromboembolism in Adults
Dosage Dosage adjustment in patients with renal impairment Half-life Reversibility Monitoring Comparisons
Unfractionated heparin*†
333 units per kg SC first dose, followed by 250 units per kg SC twice daily
No adjustment 0.5 to 2 hours
Protamine Activated partial thromboplastin time or anti–factor Xa levels
Unfractionated heparin can be monitored using the activated partial thromboplastin time with an institution-specific goal range or with anti–factor Xa levels, typically using a goal of 0.3 to 0.7 IU per mL
Unfractionated heparin vs. LMWH
Considered equally effective and safe
Unfractionated heparin may be better for patients with high bleeding risk because of short half-life and reversibility
Unfractionated heparin may be favorable in patients with CrCl < 30 mL/min/1.73 m2
LMWH has lower incidence of heparin-induced thrombocytopenia
LMWH*
Enoxaparin (Lovenox)
1 mg per kg SC every 12 hours or 1.5 mg per kg SC every 24 hours†
1 mg per kg SC every 24 hours if CrCl < 30 mL/min/1.73 m2
3 to 6 hours NA Anti–factor Xa levels in selected patients
A peak level (4 hours after the dose is given) can be measured, with a goal of 0.6 to 1 unit per mL for twice-daily enoxaparin and 1.05 units per mL for dalteparin
Unfractionated heparin vs. LMWH
Considered equally effective and safe
Unfractionated heparin may be better for patients with high bleeding risk because of short half-life and reversibility
Unfractionated heparin may be favorable in patients with CrCl < 30 mL/min/1.73 m2
LMWH has lower incidence of heparin-induced thrombocytopenia
Dalteparin (Fragmin)†200 units per kg SC once
daily
Use with caution and monitor anti–factor Xa levels in patients with CrCl < 30 mL/min/1.73 m2
3 to 5 hours NA
Tinzaparin (Innohep)
175 anti–factor Xa IU per kg SC once daily for ≥ 6 days
Contraindicated in persons 90 years and older with CrCl ≤ 60 mL/min/1.73 m2
Use with caution and monitor anti–factor Xa levels in patients with CrCl < 30 mL/min/1.73 m2
3 to 4 hours NA
Fondaparinux (Arixtra)
Weight < 111 lb (50 kg): 5 mg SC daily
Weight 111 to 220 lb (50 to 100 kg): 7.5 mg SC daily
Weight > 220 lb (100 kg): 10 mg SC daily
Use with caution in patients with CrCl 30 to 50 mL/min/1.73 m2
Contraindicated in patients with CrCl ≤ 30 mL/min/1.73 m2
18 hours NA Anti–factor Xa levels (only if fondaparinux is the reference standard for the assay)
LMWH vs. fondaparinux
Comparable effectiveness and safety
Longer half-life for fondaparinux is advantageous (daily dosing) and potentially troublesome (adverse effects and lack of reversibility)
CrCl = creatinine clearance; LMWH = low-molecular-weight heparin; NA = not available; SC = subcutaneously.
*—Begin warfarin and unfractionated heparin or LMWH on day 1.†—Unfractionated heparin and dalteparin are not approved by the U.S. Food and Drug Administration for treatment of acute deep venous thrombosis. Enoxaparin, 1.5 mg per kg daily, is not approved for outpatient management of acute deep venous thrombosis or for management of acute deep venous thrombosis in pregnant patients.
Information from:
Antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians evidence-based clinical practice guidelines. Chest. 2012;141(suppl 2).
Lovenox (enoxaparin sodium injection) for subcutaneous and intravenous use [prescribing information]. Bridgewater, N.J.: Sanofi-aventis; 2011. http://products.sanofi.us/lovenox/lovenox.html. Accessed May 25, 2012.
Innohep (tinzaparin sodium injection) [prescribing information]. Ballerup, Denmark: Leo Pharmaceutical Products; 2008. http://www.accessdata.fda. gov/drugsatfda_docs/label/2008/020484s011lbl.pdf. Accessed May 25, 2012.
Arixtra (fondaparinux sodium) solution for subcutaneous injection [prescribing information]. Research Triangle Park, N.C.: GlaxoSmithKline; 2011. http://us.gsk.com/products/assets/us_arixtra.pdf. Accessed August 1, 2012.
Outpatient Anticoagulation
Date xx, xxxx ◆ Volume xx, Number xx www.aafp.org/afp American Family Physician 3
eTable B. Unfractionated Heparin, LMWH, and Fondaparinux for Outpatient Treatment of Venous Thromboembolism in Adults
Dosage Dosage adjustment in patients with renal impairment Half-life Reversibility Monitoring Comparisons
Unfractionated heparin*†
333 units per kg SC first dose, followed by 250 units per kg SC twice daily
No adjustment 0.5 to 2 hours
Protamine Activated partial thromboplastin time or anti–factor Xa levels
Unfractionated heparin can be monitored using the activated partial thromboplastin time with an institution-specific goal range or with anti–factor Xa levels, typically using a goal of 0.3 to 0.7 IU per mL
Unfractionated heparin vs. LMWH
Considered equally effective and safe
Unfractionated heparin may be better for patients with high bleeding risk because of short half-life and reversibility
Unfractionated heparin may be favorable in patients with CrCl < 30 mL/min/1.73 m2
LMWH has lower incidence of heparin-induced thrombocytopenia
LMWH*
Enoxaparin (Lovenox)
1 mg per kg SC every 12 hours or 1.5 mg per kg SC every 24 hours†
1 mg per kg SC every 24 hours if CrCl < 30 mL/min/1.73 m2
3 to 6 hours NA Anti–factor Xa levels in selected patients
A peak level (4 hours after the dose is given) can be measured, with a goal of 0.6 to 1 unit per mL for twice-daily enoxaparin and 1.05 units per mL for dalteparin
Unfractionated heparin vs. LMWH
Considered equally effective and safe
Unfractionated heparin may be better for patients with high bleeding risk because of short half-life and reversibility
Unfractionated heparin may be favorable in patients with CrCl < 30 mL/min/1.73 m2
LMWH has lower incidence of heparin-induced thrombocytopenia
Dalteparin (Fragmin)†200 units per kg SC once
daily
Use with caution and monitor anti–factor Xa levels in patients with CrCl < 30 mL/min/1.73 m2
3 to 5 hours NA
Tinzaparin (Innohep)
175 anti–factor Xa IU per kg SC once daily for ≥ 6 days
Contraindicated in persons 90 years and older with CrCl ≤ 60 mL/min/1.73 m2
Use with caution and monitor anti–factor Xa levels in patients with CrCl < 30 mL/min/1.73 m2
3 to 4 hours NA
Fondaparinux (Arixtra)
Weight < 111 lb (50 kg): 5 mg SC daily
Weight 111 to 220 lb (50 to 100 kg): 7.5 mg SC daily
Weight > 220 lb (100 kg): 10 mg SC daily
Use with caution in patients with CrCl 30 to 50 mL/min/1.73 m2
Contraindicated in patients with CrCl ≤ 30 mL/min/1.73 m2
18 hours NA Anti–factor Xa levels (only if fondaparinux is the reference standard for the assay)
LMWH vs. fondaparinux
Comparable effectiveness and safety
Longer half-life for fondaparinux is advantageous (daily dosing) and potentially troublesome (adverse effects and lack of reversibility)
CrCl = creatinine clearance; LMWH = low-molecular-weight heparin; NA = not available; SC = subcutaneously.
*—Begin warfarin and unfractionated heparin or LMWH on day 1.†—Unfractionated heparin and dalteparin are not approved by the U.S. Food and Drug Administration for treatment of acute deep venous thrombosis. Enoxaparin, 1.5 mg per kg daily, is not approved for outpatient management of acute deep venous thrombosis or for management of acute deep venous thrombosis in pregnant patients.
Information from:
Antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians evidence-based clinical practice guidelines. Chest. 2012;141(suppl 2).
Lovenox (enoxaparin sodium injection) for subcutaneous and intravenous use [prescribing information]. Bridgewater, N.J.: Sanofi-aventis; 2011. http://products.sanofi.us/lovenox/lovenox.html. Accessed May 25, 2012.
Innohep (tinzaparin sodium injection) [prescribing information]. Ballerup, Denmark: Leo Pharmaceutical Products; 2008. http://www.accessdata.fda. gov/drugsatfda_docs/label/2008/020484s011lbl.pdf. Accessed May 25, 2012.
Arixtra (fondaparinux sodium) solution for subcutaneous injection [prescribing information]. Research Triangle Park, N.C.: GlaxoSmithKline; 2011. http://us.gsk.com/products/assets/us_arixtra.pdf. Accessed August 1, 2012.
Outpatient Anticoagulation
4 American Family Physician www.aafp.org/afp Volume xx, Number xx ◆ Date xx, xxxx
eTable C. Perioperative Management of Warfarin
Warfarin (Coumadin) indication
Risk level for VTE Bleeding risk category RecommendationMechanical heart valve Chronic atrial fibrillation VTE
At least 1 of the following:
Aortic valve prosthesis (caged-ball or tilting-disk)
Mitral valve prosthesis (any)
Stroke or TIA within past 6 months
May also include:
Patients with a history of stroke or TIA more than 3 months before surgery and a CHADS2 score < 5
Patients undergoing surgeries with high risk of thromboembolism
At least 1 of the following:
CHADS2 score of 5 or 6
Rheumatic mitral valve disease
Stroke or TIA within past 3 months
May also include:
Patients with a history of stroke or TIA more than 3 months before surgery and a CHADS2 score < 5
Patients undergoing surgeries with high risk of thromboembolism
At least 1 of the following:
Severe thrombophilia*
VTE within past 3 months
May also include:
Previous thromboembolism during temporary vitamin K antagonist interruption
Patients undergoing surgeries with high risk of thromboembolism
High (> 10% annual risk) Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning approximately 24 hours after the procedure
High‡ Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning 48 to 72 hours after the procedure
Aortic valve prosthesis (bileaflet) and at least 1 of the following: age older than 75 years; atrial fibrillation; congestive heart failure; diabetes mellitus; hypertension; prior stroke or TIA
CHADS2 score of 3 or 4 At least 1 of the following:
Active cancer§
Nonsevere thrombophilic condition||
Recurrent VTE
VTE within past 3 to 12 months
Moderate (5 to 10% annual risk)
Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low (base bridging on patient- and surgery-related factors‡)
Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Therapeutic dose of LMWH before the procedure† and beginning approximately 24 hours after the procedure
High (base bridging on patient- and surgery-related factors‡)
Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning 48 to 72 hours after the procedure
Aortic valve prosthesis (bileaflet) without atrial fibrillation and no other stroke risk factors
No prior stroke or TIA and CHADS2 score ≤ 2
Single VTE occurred > 12 months ago and no other risk factors
Low (< 5% annual risk) Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Do not bridge
High‡ Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Do not bridge
CHADS2 = congestive heart failure, hypertension, age ≥ 75 years, diabetes mellitus, prior ischemic stroke or TIA (doubled); LMWH = low-molecular-weight heparin; TIA = transient ischemic attack; VTE = venous thromboembolism.
*—Such as protein C or S deficiency, antiphospholipid antibodies, or antithrombin deficiency.†—Stop subcutaneous LMWH 24 hours before surgery.‡—Surgeries with a higher risk of bleeding include urologic surgeries, large colon polyp resection, and surgeries that involve vascular organs or have extensive tissue injury potential. Bleeding risk in hospitalized patients has been linked to multiple factors including active gastric or duodenal ulcer, bleeding within 3 months before admission, and thrombocytopenia.§—Defined as cancer treated within 6 months or palliative.||—Such as heterozygous factor V Leiden mutation.
Information from:
Antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians evidence-based clinical practice guidelines. Chest. 2012;141(suppl 2).
du Breuil AL, Umland EM. Outpatient management of anticoagulation therapy. Am Fam Physician. 2007;75(7):1031-1042.
Douketis JD. Perioperative management of patients who are receiving warfarin therapy: an evidence-based and practical approach. Blood. 2011;117(19):5044-5049.
Kaatz S, Paje D. Update in bridging anticoagulation. J Thromb Thrombolysis. 2011;31(3):259-264.
Outpatient Anticoagulation
Date xx, xxxx ◆ Volume xx, Number xx www.aafp.org/afp American Family Physician 5
eTable C. Perioperative Management of Warfarin
Warfarin (Coumadin) indication
Risk level for VTE Bleeding risk category RecommendationMechanical heart valve Chronic atrial fibrillation VTE
At least 1 of the following:
Aortic valve prosthesis (caged-ball or tilting-disk)
Mitral valve prosthesis (any)
Stroke or TIA within past 6 months
May also include:
Patients with a history of stroke or TIA more than 3 months before surgery and a CHADS2 score < 5
Patients undergoing surgeries with high risk of thromboembolism
At least 1 of the following:
CHADS2 score of 5 or 6
Rheumatic mitral valve disease
Stroke or TIA within past 3 months
May also include:
Patients with a history of stroke or TIA more than 3 months before surgery and a CHADS2 score < 5
Patients undergoing surgeries with high risk of thromboembolism
At least 1 of the following:
Severe thrombophilia*
VTE within past 3 months
May also include:
Previous thromboembolism during temporary vitamin K antagonist interruption
Patients undergoing surgeries with high risk of thromboembolism
High (> 10% annual risk) Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning approximately 24 hours after the procedure
High‡ Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning 48 to 72 hours after the procedure
Aortic valve prosthesis (bileaflet) and at least 1 of the following: age older than 75 years; atrial fibrillation; congestive heart failure; diabetes mellitus; hypertension; prior stroke or TIA
CHADS2 score of 3 or 4 At least 1 of the following:
Active cancer§
Nonsevere thrombophilic condition||
Recurrent VTE
VTE within past 3 to 12 months
Moderate (5 to 10% annual risk)
Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low (base bridging on patient- and surgery-related factors‡)
Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Therapeutic dose of LMWH before the procedure† and beginning approximately 24 hours after the procedure
High (base bridging on patient- and surgery-related factors‡)
Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
VTE prophylaxis and
Therapeutic dose of LMWH before the procedure† and beginning 48 to 72 hours after the procedure
Aortic valve prosthesis (bileaflet) without atrial fibrillation and no other stroke risk factors
No prior stroke or TIA and CHADS2 score ≤ 2
Single VTE occurred > 12 months ago and no other risk factors
Low (< 5% annual risk) Very low (minor procedures) Dental: continue warfarin with an oral prohemostatic agent or stop warfarin 2 to 3 days before procedure
Dermatologic: continue warfarin and optimize local hemostasis
Cataract: continue warfarin
Low Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Do not bridge
High‡ Stop warfarin 5 days before surgery and restart 12 to 24 hours postoperatively
Do not bridge
CHADS2 = congestive heart failure, hypertension, age ≥ 75 years, diabetes mellitus, prior ischemic stroke or TIA (doubled); LMWH = low-molecular-weight heparin; TIA = transient ischemic attack; VTE = venous thromboembolism.
*—Such as protein C or S deficiency, antiphospholipid antibodies, or antithrombin deficiency.†—Stop subcutaneous LMWH 24 hours before surgery.‡—Surgeries with a higher risk of bleeding include urologic surgeries, large colon polyp resection, and surgeries that involve vascular organs or have extensive tissue injury potential. Bleeding risk in hospitalized patients has been linked to multiple factors including active gastric or duodenal ulcer, bleeding within 3 months before admission, and thrombocytopenia.§—Defined as cancer treated within 6 months or palliative.||—Such as heterozygous factor V Leiden mutation.
Information from:
Antithrombotic therapy and prevention of thrombosis, 9th ed: American College of Chest Physicians evidence-based clinical practice guidelines. Chest. 2012;141(suppl 2).
du Breuil AL, Umland EM. Outpatient management of anticoagulation therapy. Am Fam Physician. 2007;75(7):1031-1042.
Douketis JD. Perioperative management of patients who are receiving warfarin therapy: an evidence-based and practical approach. Blood. 2011;117(19):5044-5049.
Kaatz S, Paje D. Update in bridging anticoagulation. J Thromb Thrombolysis. 2011;31(3):259-264.
Outpatient Anticoagulation
6 American Family Physician www.aafp.org/afp Volume xx, Number xx ◆ Date xx, xxxx
eTable D. Considerations for Patient Self-Testing of International Normalized Ratio
Centers for Medicare and Medicaid Services coverage includes patients:
In whom self-testing is prescribed by a physician
Taking warfarin (Coumadin) for long-term anticoagulation for venous thromboembolism, mechanical heart valves, or atrial fibrillation
Taking warfarin for at least three months before initiation of self-testing
Who do not require testing frequency greater than once weekly
Who participate in, and successfully complete, an anticoagulation education program*
Patients who may not be good self-testing candidates include those:
Who do not demonstrate monitor or instruction competency†Who will be treated with warfarin for fewer than six months
With atypical international normalized ratio target ranges
With intellectual impairment
With known drug or alcohol abuse
With language barriers that cannot be overcome with the assistance of a family member
*—This program should explain the use of the monitor, the testing procedure, and performance of quality controls, and should assess continued appropriate monitor use.†—Competency is influenced by the patient’s vision, manual dexterity, and ability to follow the monitor procedure correctly and consistently.
Information from:
Gardiner C, Williams K, Mackie IJ, Machin SJ, Cohen H. Patient self-testing is a reliable and acceptable alternative to laboratory INR monitoring. Br J Haematol. 2005;128(2):242-247.
Matchar DB, Jacobson A, Dolor R, et al.; THINRS Executive Committee and Site Inves-tigators. Effect of home testing of international normalized ratio on clinical events [published correction appears in N Engl J Med. 2011;364(1):93]. N Engl J Med. 2010;363(17):1608-1620.
Garcia-Alamino JM, Ward AM, Alonso-Coello P, et al. Self-monitoring and self-man-agement of oral anticoagulation. Cochrane Database Syst Rev. 2010;(4):CD003839.
CMS Manual System. Pub 100-04 Medicare claims processing. Prothrombin time (PT/INR) monitoring for home anticoagulation management. https://www.cms.gov/transmittals/downloads/R1562CP.pdf. Accessed August 29, 2011.